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NACA是人类红细胞分化的正向调节因子。

NACA is a positive regulator of human erythroid-cell differentiation.

作者信息

Lopez Sophie, Stuhl Laetitia, Fichelson Serge, Dubart-Kupperschmitt Anne, St Arnaud René, Galindo Jean-Rémy, Murati Anne, Berda Nicole, Dubreuil Patrice, Gomez Sophie

机构信息

UMR599 INSERM, 27 Blvd Leï Roure, 13009 Marseille, France.

出版信息

J Cell Sci. 2005 Apr 15;118(Pt 8):1595-605. doi: 10.1242/jcs.02295. Epub 2005 Mar 22.

Abstract

We have previously identified the transcript encoding NACA (the alpha chain of the nascent-polypeptide-associated complex) as a cytokine-modulated specific transcript in the human TF-1 erythroleukemic cell line. This protein was already known to be a transcriptional co-activator that acts by potentiating AP-1 activity in osteoblasts, and is known to be involved in the targeting of nascent polypeptides. In this study, we investigate the role of NACA in human hematopoiesis. Protein distribution analyses indicate that NACA is expressed in undifferentiated TF-1 cells and in human-cord-blood-derived CD34(+) progenitor cells. Its expression is maintained during in vitro erythroid differentiation but, in marked contrast, its expression is suppressed during their megakaryocytic or granulocytic differentiation. Ectopic expression of NACA in CD34(+) cells under culture conditions that induce erythroid-lineage differentiation leads to a marked acceleration of erythroid-cell differentiation. Moreover, ectopic expression of NACA induces erythropoietin-independent differentiation of TF-1 cells, whereas downregulation of NACA by RNA interference abolishes the induction of hemoglobin production in these cells and diminishes glycophorin-A (GPA) expression by CD34(+) progenitors cultured under erythroid differentiation conditions. Altogether, these results characterize NACA as a new factor involved in the positive regulation of human erythroid-cell differentiation.

摘要

我们之前已将编码NACA(新生多肽相关复合物的α链)的转录本鉴定为人类TF-1红白血病细胞系中一种细胞因子调节的特异性转录本。已知该蛋白是一种转录共激活因子,通过增强成骨细胞中的AP-1活性发挥作用,并且已知其参与新生多肽的靶向作用。在本研究中,我们探究了NACA在人类造血过程中的作用。蛋白质分布分析表明,NACA在未分化的TF-1细胞和人脐带血来源的CD34(+)祖细胞中表达。在体外红系分化过程中其表达得以维持,但与之形成鲜明对比的是,在巨核细胞或粒细胞分化过程中其表达受到抑制。在诱导红系谱系分化的培养条件下,NACA在CD34(+)细胞中的异位表达导致红系细胞分化显著加速。此外,NACA的异位表达诱导TF-1细胞发生不依赖促红细胞生成素的分化,而通过RNA干扰下调NACA可消除这些细胞中血红蛋白生成的诱导作用,并减少在红系分化条件下培养的CD34(+)祖细胞中血型糖蛋白A(GPA)的表达。总之,这些结果表明NACA是参与人类红系细胞分化正调控的一个新因子。

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